Identifying dementia outcomes in UK Biobank: a validation study of primary care, hospital admissions and mortality data

Tim Wilkinson,Deborah Bathgate,Cathie L M Sudlow,Chris Lerpiniere,Kristiina Rannikmäe,Suvankar Pal,John T O’Brien,David E Henshall,Kathryn Bush,Robin Flaig,Christian Schnier,Naomi E Allen,Tom C Russ

doi:10.1007/s10654-019-00499-1

Abstract

Prospective, population-based studies that recruit participants in mid-life are valuable resources for dementia research. Follow-up in these studies is often through linkage to routinely-collected healthcare datasets. We investigated the accuracy of these datasets for dementia case ascertainment in a validation study using data from UK Biobank—an open access, population-based study of > 500,000 adults aged 40–69 years at recruitment in 2006–2010. From 17,198 UK Biobank participants recruited in Edinburgh, we identified those with ≥ 1 dementia code in their linked primary care, hospital admissions or mortality data and compared their coded diagnoses to clinical expert adjudication of their full-text medical record. We calculated the positive predictive value (PPV, the proportion of cases identified that were true positives) for all-cause dementia, Alzheimer’s disease and vascular dementia for each dataset alone and in combination, and explored algorithmic code combinations to improve PPV. Among 120 participants, PPVs for all-cause dementia were 86.8%, 87.3% and 80.0% for primary care, hospital admissions and mortality data respectively and 82.5% across all datasets. We identified three algorithms that balanced a high PPV with reasonable case ascertainment. For Alzheimer’s disease, PPVs were 74.1% for primary care, 68.2% for hospital admissions, 50.0% for mortality data and 71.4% in combination. PPV for vascular dementia was 43.8% across all sources. UK routinely-collected healthcare data can be used to identify all-cause dementia in prospective studies. PPVs for Alzheimer’s disease and vascular dementia are lower. Further research is required to explore the geographic generalisability of these findings.

Highlights

Dementia is a growing public health concern worldwide [1], and prospective, population-based studies are necessary to improve our understanding of its natural history and risk factors.UK Biobank (UKB, www.ukbiobank.ac.uk) is a very large, prospective, population-based cohort study that was established to facilitate research into the determinants of health and disease, primarily in middle and old age [2]
We aimed to estimate the positive predictive value (PPV) of dementia coding in UK primary care, hospital admissions and national mortality datasets alone and in combination using data from UKB
We identified UK Biobank participants recruited in Edinburgh, Scotland, who had ≥ 1 dementia code in their linked

Summary

Introduction

Dementia is a growing public health concern worldwide [1], and prospective, population-based studies are necessary to improve our understanding of its natural history and risk factors. UK Biobank (UKB, www.ukbiobank.ac.uk) is a very large, prospective, population-based cohort study that was established to facilitate research into the determinants of health and disease, primarily in middle and old age [2]. UKB collected a wealth of exposure sociodemographic, lifestyle, environmental and health information during the baseline assessment, along with a range of physical measures and cognitive testing. UKB has approved projects to study dementia and cognitive disorders across a wide range of topics, including: identifying genetic, environmental and lifestyle risk factors for dementia; establishing the relationship between neuroimaging findings and cognition and developing dementia risk prediction models (www.ukbiobank.ac.uk/approved-research)

Objectives

Methods

Results

Conclusion